钙通道阻滞剂对大鼠门静脉钙依赖性收缩的影响。
Effects of calcium entry blockers on calcium-dependent contractions of rat portal vein.
作者信息
Dacquet C, Mironneau C, Mironneau J
机构信息
Institut de Biochimie Cellulaire et Neurochimie du CNRS, Université de Bordeaux II, France.
出版信息
Br J Pharmacol. 1987 Sep;92(1):203-11. doi: 10.1111/j.1476-5381.1987.tb11313.x.
1 The effects of six calcium entry blockers belonging to the dihydropyridine (isradipine or PN 200-110, nifedipine, nicardipine), verapamil (D888 or desmethoxyverapamil, D600 or gallopamil) and diltiazem classes were investigated on isometric spontaneous contractions and contractions induced by high-K+ solutions, noradrenaline, acetylcholine and caffeine. 2 The rank order of potency was PN 200-110 greater than nicardipine = nifedipine = D888 greater than D600 greater than diltiazem from experiments on spontaneous contractions and high-K+ induced contractions. With depolarized preparations, the concentration-response curves for nicardipine, PN 200-110, nifedipine and D600 were significantly shifted to the left indicating that the calcium entry blockers show voltage-dependent inhibitory properties. This effect was not significant with D888 and diltiazem. 3 All the calcium entry blockers strongly reduced the noradrenaline (NA)- and acetylcholine (ACh)-induced contractions at concentrations which produced complete inhibition of spontaneous contractions. They had a slight effect on caffeine-induced contractions. 4 In Ca2+-free, EGTA-containing solutions, both ACh, NA and caffeine produced transient contractions, the amplitude of which could be taken as a measurement of the amount of internal calcium present in a drug-sensitive calcium store. The filling of the calcium store was maximal after 10-12 min of calcium loading in 2.1 mM Ca2+, while the depletion was complete after 4-6 min of perfusion in Ca2+-free solution. 5 At concentrations which abolished spontaneous contractions, PN 200-110, nifedipine, D888 and D600 had no appreciable effect on contractions evoked in Ca2+-free solutions by ACh, NA and caffeine. When added in Ca2+-containing solutions diltiazem and, to a lesser extent, nicardipine strongly reduced the contractions evoked in Ca2 -free solutions, suggesting that they inhibited the filling of the internal calcium store. 6. These results indicate that the six calcium entry blockers are potent inhibitors of calcium influx through voltage-dependent calcium channels. Two of them (diltiazem and nicardipine) may exert an additional effect to depress contractions dependent on intracellular calcium release.
- 研究了属于二氢吡啶类(伊拉地平或PN 200 - 110、硝苯地平、尼卡地平)、维拉帕米类(D888或去甲氧基维拉帕米、D600或加洛帕米)和地尔硫䓬类的六种钙通道阻滞剂对等长自发收缩以及由高钾溶液、去甲肾上腺素、乙酰胆碱和咖啡因诱导的收缩的影响。2. 从自发收缩和高钾诱导收缩的实验来看,效力的排序为PN 200 - 110大于尼卡地平 = 硝苯地平 = D888大于D600大于地尔硫䓬。对于去极化的标本,尼卡地平、PN 200 - 110、硝苯地平和D600的浓度 - 反应曲线显著左移,表明钙通道阻滞剂具有电压依赖性抑制特性。D888和地尔硫䓬的这种效应不显著。3. 所有钙通道阻滞剂在产生完全抑制自发收缩的浓度下,都能强烈降低去甲肾上腺素(NA)和乙酰胆碱(ACh)诱导的收缩。它们对咖啡因诱导的收缩有轻微影响。4. 在无钙、含乙二醇双乙醚二胺四乙酸(EGTA)的溶液中,ACh、NA和咖啡因都会产生短暂收缩,其幅度可作为药物敏感钙库中存在的细胞内钙量的一种度量。在2.1 mM钙中加载钙10 - 12分钟后,钙库的充盈达到最大,而在无钙溶液中灌注4 - 6分钟后,钙库耗尽完全。5. 在消除自发收缩的浓度下,PN 200 - 110、硝苯地平、D888和D600对无钙溶液中由ACh、NA和咖啡因诱发的收缩没有明显影响。当加入含钙溶液中时,地尔硫䓬以及在较小程度上尼卡地平强烈降低无钙溶液中诱发的收缩,表明它们抑制细胞内钙库的充盈。6. 这些结果表明,六种钙通道阻滞剂是通过电压依赖性钙通道抑制钙内流的有效抑制剂。其中两种(地尔硫䓬和尼卡地平)可能还具有额外作用,以抑制依赖细胞内钙释放的收缩。
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